Evolutionarily divergentMycobacterium tuberculosisCTP synthase filaments are under selective pressure

Author:

Lynch Eric M.ORCID,Lu Yao,Park Jin Ho,Shao Lin,Kollman JustinORCID,Rego E. HesperORCID

Abstract

ABSTRACTThe final and rate-limiting enzyme in pyrimidine biosynthesis, CTP synthase (CTPS), is essential for the viability ofMycobacterium tuberculosisand other mycobacteria. Its product, CTP, is critical for RNA, DNA, lipid and cell wall synthesis, and is involved in chromosome segregation. In various organisms across the tree of life, CTPS assembles into higher-order filaments, leading us to hypothesize thatM. tuberculosisCTPS (mtCTPS) also forms higher-order structures. Here, we show that mtCTPS does assemble into filaments but with an unusual architecture not seen in other organisms. Through a combination of structural, biochemical, and cellular techniques, we show that polymerization stabilizes the active conformation of the enzyme and resists product inhibition, potentially allowing for the highly localized production of CTP within the cell. Indeed, CTPS filaments localize near the CTP-dependent complex needed for chromosome segregation, and cells expressing mutant enzymes unable to polymerize are altered in their ability to robustly form this complex. Intriguingly, mutants that alter filament formation are under positive selection in clinical isolates ofM. tuberculosis, pointing to a critical role needed to withstand pressures imposed by the host and/or antibiotics. Taken together, our data reveal an unexpected mechanism for the spatially organized production of a critical nucleotide inM. tuberculosis, which may represent a vulnerability of the pathogen that can be exploited with chemotherapy.

Publisher

Cold Spring Harbor Laboratory

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